Dose response kinetics of CD8 lymphocytes from young animals transfused into old animals and challenged with influenza

Richard Aspinall,Sheila Govind,Pierre Olivier Lang,Antonio Lapenna

doi:10.1186/1742-4933-10-34

Richard Aspinall, Sheila Govind + Show 2 more

Open Access

https://doi.org/10.1186/1742-4933-10-34

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Journal: Immunity & Ageing	Publication Date: Aug 16, 2013
Citations: 32	License type: CC BY 2.0

Affiliation: Cranfield University, Clinique de Genolier

Abstract

Transfusion of autologous leukocytes after prolonged storage has been proposed as a means of rejuvenating the immune system of older individuals. The rationale for this approach is that age related immune decline is associated with a diminished pool of naïve T cells following atrophy of the thymus and reduction in thymic output. The presence of high levels of naïve T cells within the blood of young individuals could provide a boost to the immune system of an older “self” through a rejuvenation of the naïve T cell pool. However what remains unresolved is whether the cells could be incorporated effectively into the T cell pool of the host and whether effectors could be generated. Using CD45 congenic mice in our experiments we show that the transfusion of young donor cells into older congenic host animals leads to their successful incorporation into the peripheral T cell pool. When the recipients were challenged with influenza virus, specific effector CD8 cells were generated which were of both host and donor origin. We found no relationship between the number of responder cells of donor origin at the time of assay and the number of cells injected.

Highlights

Influenza is an infectious disease of limited duration in young adults with an optimal functioning immune system
Young blood leukocyte constituents Analysis of the blood collected from young animals revealed that the mononuclear leukocyte population contained 65% CD3+ cells of which 33% were CD8+
This study reveals that cells from young animals transferred to an older congenic host can be incorporated into the peripheral T lymphocyte pool without having a significant effect on the total number of CD3+ T cells

Summary

Introduction

Influenza is an infectious disease of limited duration in young adults with an optimal functioning immune system. Epidemiological studies reveal that the prevalence of diseases affecting epithelial barriers, such as respiratory and Improvements in the CD8 T cell pool of old animals, can be achieved by increasing the number of reactive cells through adoptive transfer. This was tested in a recent study using virus-specific transgenic CD8 T cells taken from young animals, and transfused into old animals. One option which has been proposed is to increase the number of naive T lymphocytes in the peripheral T cell pool by transfusion [18] This could be achieved by the preservation of quantities of an individual’s blood leukocytes at a younger age, which would be transfused back into them at a later stage, when the immune system demonstrates some features of immunosenescence. The transfer of syngeneic or autochthonous T cells from young to old whilst having been suggested [18] has not been tested

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